Molecular Pathways: Harnessing E2F1 Regulation for Prosenescence Therapy in p53-Defective Cancer Cells

Laine, Antti; Westermarck, Jukka

doi:10.1158/1078-0432.ccr-13-1942

Cited by 31 publications

(25 citation statements)

References 69 publications

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“…2 ). These findings coincide with known effects of other MDM2 inhibitors on the p53/MDM2/ PUMA/p21/pRb/E2F1 cascade [12,45,46] . Further p53-mediated downstream effects alter the p53/MDM2/ PUMA/p21/pRb/E2F1 cascade and mediate the antitumoral effects of MDM2 inhibitors [12,35,46] .…”

Section: The Mdm2 Inhibitor Nvp-cgm097 Increases the Expression Of P5supporting

confidence: 88%

“…These findings indicate that NVP-CGM097 is a highly specific MDM2 inhibitor increasing p53, PUMA, and p21 expression and interacting with the MDM2/p53/PUMA/p21/Rb/E2F1 cascade [46] . CDK4/6-cyclin D-or CDK2-cyclin E-mediated phosphorylation of Rb protein results in its inactivation, dissociation of the pRb/E2F complex, and repression of E2F transcription factors [46,80] . Double knockout experiments in Men1+/-Cdk4-/-mice indicate that CDK4 is essential for NET development [81] .…”

Section: Discussionmentioning

confidence: 78%

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The HDM2 (MDM2) Inhibitor NVP-CGM097 Inhibits Tumor Cell Proliferation and Shows Additive Effects with 5-Fluorouracil on the p53-p21-Rb-E2F1 Cascade in the p53<sup>wild type</sup> Neuroendocrine Tumor Cell Line GOT1

et al. 2016

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Background/Aims: The tumor suppressor p53 is depleted in many tumor cells by the E3 ubiquitin ligase mouse double minute 2 homolog (MDM2) through MDM2/p53 interaction. A novel target for inhibiting p53 degradation and for causing reexpression of p53^{wild type} is inhibition of MDM2. The small molecule NVP-CGM097 is a novel MDM2 inhibitor. We investigated MDM2 inhibition as a target in neuroendocrine tumor cells in vitro. Methods: Human neuroendocrine tumor cell lines from the pancreas (BON1), lung (NCI-H727), and midgut (GOT1) were incubated with the MDM2 inhibitor NVP-CGM097 (Novartis) at concentrations from 4 to 2,500 nM. Results: While p53^{wild type} GOT1 cells were sensitive to NVP-CGM097, p53^mutated BON1 and p53^mutated NCI-H727 cells were resistant to NVP-CGM097. Incubation of GOT1 cells with NVP-CGM097 at 100, 500, and 2,500 nM for 96 h caused a significant decline in cell viability to 84.9 ± 9.2% (p < 0.05), 77.4 ± 6.6% (p < 0.01), and 47.7 ± 9.2% (p < 0.01). In a Western blot analysis of GOT1 cells, NVP-CGM097 caused a dose-dependent increase in the expression of p53 and p21 tumor suppressor proteins and a decrease in phospho-Rb and E2F1. Experiments of co-incubation of NVP-CGM097 with 5-fluorouracil, temozolomide, or everolimus each showed additive antiproliferative effects in GOT1 cells. NVP-CGM097 and 5-fluorouracil increased p53 and p21 expression in an additive manner. Conclusions: MDM2 inhibition seems a promising novel therapeutic target in neuroendocrine tumors harboring p53^{wild type}. Further investigations should examine the potential role of MDM2 inhibitors in neuroendocrine tumor treatment.

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Section: The Mdm2 Inhibitor Nvp-cgm097 Increases the Expression Of P5supporting

confidence: 88%

Section: Discussionmentioning

confidence: 78%

The HDM2 (MDM2) Inhibitor NVP-CGM097 Inhibits Tumor Cell Proliferation and Shows Additive Effects with 5-Fluorouracil on the p53-p21-Rb-E2F1 Cascade in the p53<sup>wild type</sup> Neuroendocrine Tumor Cell Line GOT1

et al. 2016

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“…Its protein expression level is increased in many human cancers such as hepatocarcinomas, digestive adenocarcinomas and ovarian cancers, and its downregulation in p53- and RB-compromised cancer cells can trigger their senescence. 1 Further understanding of E2F1 expression regulation would help to develop strategies targeting this protein in cancer cells.…”

mentioning

confidence: 99%

DNA damage and S phase-dependent E2F1 stabilization requires the cIAP1 E3-ubiquitin ligase and is associated with K63-poly-ubiquitination on lysine 161/164 residues

et al. 2017

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The E2F transcription factor 1 is subtly regulated along the cell cycle progression and in response to DNA damage by post-translational modifications. Here, we demonstrated that the E3-ubiquitin ligase cellular inhibitor of apoptosis 1 (cIAP1) increases E2F1 K63-poly-ubiquitination on the lysine residue 161/164 cluster, which is associated with the transcriptional factor stability and activity. Mutation of these lysine residues completely abrogates the binding of E2F1 to CCNE, TP73 and APAF1 promoters, thus inhibiting transcriptional activation of these genes and E2F1-mediated cell proliferation control. Importantly, E2F1 stabilization in response to etoposide-induced DNA damage or during the S phase of cell cycle, as revealed by cyclin A silencing, is associated with K63-poly-ubiquitinylation of E2F1 on lysine 161/164 residues and involves cIAP1. Our results reveal an additional level of regulation of the stability and the activity of E2F1 by a non-degradative K63-poly-ubiquitination and uncover a novel function for the E3-ubiquitin ligase cIAP1.

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“…Furthermore, Ror2 is expressed highly in embryonic tissues that contain abundantly proliferating cells, indicating that E2F1‐induced transcriptional activation of Ror2 might also be involved in the expression of Ror2 in these proliferating cells during embryogenesis. E2F1 is also activated strongly in cancer cells through various mechanisms, including activation of oncogenes and inhibition of tumor suppressor genes . It has been shown that Ror2 is expressed highly in lung adenocarcinoma cells harboring p53 loss‐of‐function mutations and in human papillomavirus (HPV)‐positive head and neck squamous cell carcinoma, where HPV oncogenic protein E7 represses Rb .…”

Section: Discussionmentioning

confidence: 99%

E2F1‐Ror2 signaling mediates coordinated transcriptional regulation to promote G1/S phase transition in bFGF‐stimulated NIH/3T3 fibroblasts

2020

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Ror2 signaling has been shown to regulate the cell cycle progression in normal and cancer cells. However, the molecular mechanism of the cell cycle progression upon activation of Ror2 signaling still remains unknown. Here, we found that the expression levels of Ror2 in G1‐arrested NIH/3T3 fibroblasts are low and are rapidly increased following the cell cycle progression induced by basic fibroblast growth factor (bFGF) stimulation. By expressing wild‐type or a dominant negative mutant of E2F1, we show that E2F1 mediates bFGF‐induced expression of Ror2, and that E2F1 binds to the promoter of the Ror2 gene to activate its expression. We also found that G1/S phase transition of bFGF‐stimulated NIH/3T3 cells is delayed by the suppressed expression of Ror2. RNA‐seq analysis revealed that the suppressed expression of Ror2 results in the decreased expression of various E2F target genes concomitantly with increased expression of Forkhead box O (FoxO) target genes, including p21Cip1, and p27Kip1. Moreover, the inhibitory effect of Ror2 knockdown on the cell cycle progression can be restored by suppressed expression of p21Cip1, p27Kip1,or FoxO3a. Collectively, these findings indicate that E2F1‐Ror2 signaling mediates the transcriptional activation and inhibition of E2F1‐driven and FoxO3a‐driven cell cycle‐regulated genes, respectively, thereby promoting G1/S phase transition of bFGF‐stimulated NIH/3T3 cells.

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Molecular Pathways: Harnessing E2F1 Regulation for Prosenescence Therapy in p53-Defective Cancer Cells

Cited by 31 publications

References 69 publications

The HDM2 (MDM2) Inhibitor NVP-CGM097 Inhibits Tumor Cell Proliferation and Shows Additive Effects with 5-Fluorouracil on the p53-p21-Rb-E2F1 Cascade in the p53<sup>wild type</sup> Neuroendocrine Tumor Cell Line GOT1

The HDM2 (MDM2) Inhibitor NVP-CGM097 Inhibits Tumor Cell Proliferation and Shows Additive Effects with 5-Fluorouracil on the p53-p21-Rb-E2F1 Cascade in the p53<sup>wild type</sup> Neuroendocrine Tumor Cell Line GOT1

DNA damage and S phase-dependent E2F1 stabilization requires the cIAP1 E3-ubiquitin ligase and is associated with K63-poly-ubiquitination on lysine 161/164 residues

E2F1‐Ror2 signaling mediates coordinated transcriptional regulation to promote G1/S phase transition in bFGF‐stimulated NIH/3T3 fibroblasts

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